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Effect of antibiotics on certain aspects of bacteriophage SP-15 development in Bacillus subtilis W23.

机译:抗生素对枯草芽孢杆菌W23中噬菌体SP-15发育的某些方面的影响。

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Bacillus subtilis W23 was infected with bacteriophage SP-15. Two waves of phage-specific RNA synthesis were observed. Wave I was prereplicative, and wave II was coincident with replication of the viral genome. To determine the temporal appearance of general classes of phage-coded messengers and proteins, we studied the dependence of lysozyme synthesis, phage production, and DNA synthesis on time of addition of transcriptional and translational inhibitors. Lysozyme synthesis started to become refractile to a variety of transcriptional inhibitors (rifampin, streptolydigin, and actinomycin D) between 20 and 22 min postinfection and was completely refractile by 30 min. Nevertheless, functional enzyme did not appear until 45 to 47 min postinfection; lysozyme was maximal by 65 min. Rna isolated from SP-15 phage-infected cells was used to program the cell-free synthesis of lysozyme. The messenger was synthesized exclusively between 20 and 30 min postinfection. Lysozyme messengers were stable. The data imply that lysozyme messengers were present 52 min prior to their translation. Progeny virus formation remained sensitive to transcriptional inhibitors until 40 to 50 min postinfection, and sensitivity to chloramphenicol lasted 65 min. The first progeny viruses appeared at 75 min. Again, an unusually long lag between completion of functional messengers and their translation was evident. The aforementioned data indicated that transcription of lysozyme messengers and, at least, some messengers, whose products are essential for phage production, are uniquely associated with waves I and II of RNA synthesis, respectively. However, messengers whose products are essential for normal amounts of DNA synthesis were apparently synthesized during both waves; transcription of these messengers was transiently repressed (using the term broadly) between 30 and 40 min postinfection. Judging from the dependence of DNA synthesis on time of chloramphenicol addition, proteins essential for normal amounts of DNA synthesis were also synthesized in two discrete waves, each yielding sufficient protein for half-maximal levels of DNA synthesis. An hiatus in the synthesis of the proteins in question was evident between 45 and 65 min postinfection; evidence cited in this paper indicates that this hiatus did not result from messenger depletion, which, in turn, implied some type of translational-level control. This latter conclusion is substantiated by the lysozyme synthesis that occurred during the same interval when synthesis of certain proteins for DNA replication was transiently repressed.
机译:枯草芽孢杆菌W23被噬菌体SP-15感染。观察到两波噬菌体特异性RNA合成。 Wave I具有前进性,波浪II与病毒基因组的复制一致。为了确定一般类别的噬菌体编码信使和蛋白质的时间外观,我们研究了溶菌酶合成,噬菌体生产和DNA合成的依赖性在添加转录和平移抑制剂时。溶菌酶合成开始变成各种转录抑制剂(利福平,链霉蛋白和放线霉素D)在20至22分钟之间的各种转录抑制剂(Lifampin,Streptolydigin,并且在30分钟内完全折射。然而,功能性酶直到45至47分钟的发射;溶菌酶最大65分钟。从SP-15噬菌体感染的细胞分离的RNA用于编程无细胞的合成溶菌酶。信使专门合成20至30分钟的繁殖。溶菌酶使者是稳定的。数据意味着在翻译之前的溶菌酶传染率为52分钟。后代病毒形成对转录抑制剂保持敏感,直至40〜50分钟的发射后染色,对氯霉素的敏感性持续65分钟。第一个后代病毒出现在75分钟。同样,在完成功能使者和他们的翻译之间的异常长期滞后是显而易见的。上述数据表明,溶菌酶传道人的转录,并且至少有一些传道人,其产品对于噬菌体生产是必不可少的,它们分别与RNA合成的波浪I和II唯一相关。然而,在两波浪期间显然合成了其产品对正常DNA合成必不可少的信使;这些信使的转录瞬时压抑(使用术语广泛使用)在30到40分钟之间进行营收。从DNA合成的依赖性判断在氯霉素的时间中,在两个离散的波中也合成了正常量DNA合成的蛋白质,每个DNA合成都是足够的蛋白质,用于半最大水平的DNA合成。在问题中合成的中断是明显的,在45%至65分钟之间是明显的;本文引用的证据表明,这种中断不会因信使耗尽而导致,反过来暗示了某种类型的翻译级控制。后一种结论是通过在相同的间隔期间发生的溶菌酶合成证实,当某些蛋白质的用于DNA复制的合成时是瞬时压抑的。

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